CA2276921A1 - Manufacture of d,1-alpha-tocopherol - Google Patents
Manufacture of d,1-alpha-tocopherol Download PDFInfo
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- CA2276921A1 CA2276921A1 CA002276921A CA2276921A CA2276921A1 CA 2276921 A1 CA2276921 A1 CA 2276921A1 CA 002276921 A CA002276921 A CA 002276921A CA 2276921 A CA2276921 A CA 2276921A CA 2276921 A1 CA2276921 A1 CA 2276921A1
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D311/00—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only hetero atom, condensed with other rings
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- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D311/00—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only hetero atom, condensed with other rings
- C07D311/02—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only hetero atom, condensed with other rings ortho- or peri-condensed with carbocyclic rings or ring systems
- C07D311/04—Benzo[b]pyrans, not hydrogenated in the carbocyclic ring
- C07D311/58—Benzo[b]pyrans, not hydrogenated in the carbocyclic ring other than with oxygen or sulphur atoms in position 2 or 4
- C07D311/70—Benzo[b]pyrans, not hydrogenated in the carbocyclic ring other than with oxygen or sulphur atoms in position 2 or 4 with two hydrocarbon radicals attached in position 2 and elements other than carbon and hydrogen in position 6
- C07D311/72—3,4-Dihydro derivatives having in position 2 at least one methyl radical and in position 6 one oxygen atom, e.g. tocopherols
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Abstract
A process for the manufacture of d,l-.alpha.-tocopherol by the acid-catalyzed condensation of trimethylhydroquinone with isophytol or phytol in ethylene or propylene carbonate or a mixture of both carbonates, or in a mixture of one or both of the carbonates and a non-polar solvent, comprises carrying out the condensation in the presence of at most 0.4 weight percent based on the weight of isophytol or phytol of 12-tungstophosphoric acid, 12-molybdophosphoric acid or 12-tungstosilicic acid. The product of the process is the most active and industrially important member of the vitamin E group.
Description
Case 20168 The present invention is concerned with a novel process for the manu-s facture of d,l-a-tocopherol by the acid-catalyzed condensation of trimethyl-hydroquinone (TMH(a) with isophytol (IP) or phytol (PH) in a solvent. As is known, d,l-a-tocopherol is a diastereoisomeric mixture of 2,5,7,8-tetramethyl-2-(4',8',12'-trimethyl-tridecyl)-6-chromanol (a-tocopherol), which is the most active and industrially most important member of the vitamin E group.
to Many processes for the manufacture of d,l-a-tocopherol by the conden-sation of TMHQ with IP or PH in the presence of a catalyst or catalyst system and in a solvent or solvent system are described in the literature. These processes go back to the work of Karrer et al., Bergel et al. as well as Smith et is al. [see Helv. Chim. Acta 21, 520 et seq. (1938), Nature 142, 36 et seq.
(1938) and, respectively, Science 88, 37 et seq. (1938) and J. Am. Chem. Soc. 61, et seq. (1939)]. While Karrer et al. carried out the synthesis of d,l-a-tocopherol from TMHII and phytyl bromide in the presence of anhydrous zinc chloride (ZnClz; a Lewis acid), not only Bergel et al. but also Smith et al. used TMHQ
2o and PH as starting materials. In the following years mainly modifications, e.g. alternative solvents and Lewis acids, were developed. From the work of Karrer et al. there was developed in the year 1941 a technically interesting process for the manufacture of d,l-a-tocopherol which was based on the condensation of TMH(~,l with IP in the presence of the catalyst system 25 ZnClz/hydrochloric acid (HCl) (US Patent 2 411 969). Later publications, e.g.
Japanese Patent Publications (Kokai) 54380/1985, 64977/1985 and 226979/1987 [Chemical Abstracts (C.A.) 103, 123731s (1985), C.A. 103, 104799d (1985) and, respectively, C.A. 110, 39217r (1989)], describe this condensation in the presence of zinc and/or ZnCl2 and a Bronsted (protonic) 3o acid, such as a hydrohalic acid, e.g. HC1, trichloroacetic acid, acetic acid and the like, especially ZnCl2/HCl, as the catalyst system. Disadvantages of these Pa/vs 7.4.1999 _2_ and further published processes featuring ZnCl2 in combination with a Bronsted acid are the corrosive properties of the acids and the contamination of the waste water with zinc ions as a result of the large amount of ZnCl2 required for the catalysis.
The manufacture of d,l-a-tocopherol by the reaction of TMHQ with phytyl chloride, PH or IP in the presence of boron trifluoride (BF3) or its etherate (BF3~Et20) is described in German Patents 960720 and 1015446 as well as in US Patent 3 444 213. However BF3 too has corrosive properties.
Also, the condensation of TMHQ with IP or PH in the presence of a Lewis acid, e.g. ZnCl2, BF3 or aluminium trichloride (A1C13), a strong acid, e.g.
HCI, and an amine salt as the catalyst system is described in European Patent Publication (EP) 100471. In an earlier patent publication, DOS 2606830, the IP or PH is pretreated with ammonia or an amine before the condensation with TMHQ in the presence of ZnCl2 and an acid is effected. In both cases corrosion problems occur.
A further interesting method for the manufacture of d,l-a-tocopherol 2o from TMHQ and IP comprises using an isolated TMHfa-BF3 or -A1C13 complex and a solvent mixture featuring a nitro compound (DOS 1909164). This process avoids to a large extent the formation of undesired by-products because it involves mild reaction conditions. The yield of d,l-a-tocopherol, based on IP and the use of the solvent mixture methylene chloride/nitro-methane, is given as 77%. However, the use of such a solvent mixture is disadvantageous.
The manufacture of d,l-a-tocopherol by the condensation of TMHQ with IP using cation exchange resin complexes of metal ions (Zn2+, Sn2+ and Sn4+) 3o is disclosed in Bull. Chem. Soc. Japan 50, 2477-2478 (1977); amongst other disadvantages it gives the product in unsatisfactory yields.
to Many processes for the manufacture of d,l-a-tocopherol by the conden-sation of TMHQ with IP or PH in the presence of a catalyst or catalyst system and in a solvent or solvent system are described in the literature. These processes go back to the work of Karrer et al., Bergel et al. as well as Smith et is al. [see Helv. Chim. Acta 21, 520 et seq. (1938), Nature 142, 36 et seq.
(1938) and, respectively, Science 88, 37 et seq. (1938) and J. Am. Chem. Soc. 61, et seq. (1939)]. While Karrer et al. carried out the synthesis of d,l-a-tocopherol from TMHII and phytyl bromide in the presence of anhydrous zinc chloride (ZnClz; a Lewis acid), not only Bergel et al. but also Smith et al. used TMHQ
2o and PH as starting materials. In the following years mainly modifications, e.g. alternative solvents and Lewis acids, were developed. From the work of Karrer et al. there was developed in the year 1941 a technically interesting process for the manufacture of d,l-a-tocopherol which was based on the condensation of TMH(~,l with IP in the presence of the catalyst system 25 ZnClz/hydrochloric acid (HCl) (US Patent 2 411 969). Later publications, e.g.
Japanese Patent Publications (Kokai) 54380/1985, 64977/1985 and 226979/1987 [Chemical Abstracts (C.A.) 103, 123731s (1985), C.A. 103, 104799d (1985) and, respectively, C.A. 110, 39217r (1989)], describe this condensation in the presence of zinc and/or ZnCl2 and a Bronsted (protonic) 3o acid, such as a hydrohalic acid, e.g. HC1, trichloroacetic acid, acetic acid and the like, especially ZnCl2/HCl, as the catalyst system. Disadvantages of these Pa/vs 7.4.1999 _2_ and further published processes featuring ZnCl2 in combination with a Bronsted acid are the corrosive properties of the acids and the contamination of the waste water with zinc ions as a result of the large amount of ZnCl2 required for the catalysis.
The manufacture of d,l-a-tocopherol by the reaction of TMHQ with phytyl chloride, PH or IP in the presence of boron trifluoride (BF3) or its etherate (BF3~Et20) is described in German Patents 960720 and 1015446 as well as in US Patent 3 444 213. However BF3 too has corrosive properties.
Also, the condensation of TMHQ with IP or PH in the presence of a Lewis acid, e.g. ZnCl2, BF3 or aluminium trichloride (A1C13), a strong acid, e.g.
HCI, and an amine salt as the catalyst system is described in European Patent Publication (EP) 100471. In an earlier patent publication, DOS 2606830, the IP or PH is pretreated with ammonia or an amine before the condensation with TMHQ in the presence of ZnCl2 and an acid is effected. In both cases corrosion problems occur.
A further interesting method for the manufacture of d,l-a-tocopherol 2o from TMHQ and IP comprises using an isolated TMHfa-BF3 or -A1C13 complex and a solvent mixture featuring a nitro compound (DOS 1909164). This process avoids to a large extent the formation of undesired by-products because it involves mild reaction conditions. The yield of d,l-a-tocopherol, based on IP and the use of the solvent mixture methylene chloride/nitro-methane, is given as 77%. However, the use of such a solvent mixture is disadvantageous.
The manufacture of d,l-a-tocopherol by the condensation of TMHQ with IP using cation exchange resin complexes of metal ions (Zn2+, Sn2+ and Sn4+) 3o is disclosed in Bull. Chem. Soc. Japan 50, 2477-2478 (1977); amongst other disadvantages it gives the product in unsatisfactory yields.
The use of macroreticular ion exchangers, e.g. Amberlyst~ 15, as the catalyst for the condensation of TMHQ with IP is described in US Patent 3459773. However, the d,l-a-tocopherol could not be obtained in the requisite purity.
EP 603695 describes the manufacture of d,l-a-tocopherol in liquid or supercritical carbon dioxide by the condensation of TMH~,I with IP or PH in the presence of acidic catalysts, such as ZnClz/HCl and ion exchangers. The reported yields are unsatisfactory.
to The condensation in the presence of a catalyst system which consists of iron(II) chloride, metallic iron and HCl gas or aqueous solution is described in DOS 2160103 and US Patent 3789086. The formation of less by-products is advantageous compared with the aforementioned process using ZnCh/I-ICl.
However, corrosion problems and chloride contamination are equally disadvantageous.
An interesting alternative for the condensation of TMHQ with IP to d,l-a-tocopherol comprises using trifluoroacetic acid or its anhydride as the 2o catalyst (EP 12824). Although in this process the avoidance of HCl is achieved, the catalyst is relatively expensive.
The use of the heteropoly acid 12-tungstophosphoric or 12-tungstosilicic acid as the catalyst for the condensation of TMHQ with IP was described for the first time in React. Kinet. Catal. Lett. 47(1), 59-64 (1992). d,l-a-Tocopherol could be obtained, using various solvents, in about 90% yield.
A further process described in the literature [EP 658552; Bull. Chem.
Soc. Japan 68, 3569-3571 (1995)] for the synthesis of d,l-a-tocopherol is based on the use of a scandium, yttrium or lanthanide fluorosulphonate, nitrate or sulphate, e.g. scandium trifluoromethanesulphonate. With up to about 10%
excess of IP this process gives yields up to 98%.
EP 603695 describes the manufacture of d,l-a-tocopherol in liquid or supercritical carbon dioxide by the condensation of TMH~,I with IP or PH in the presence of acidic catalysts, such as ZnClz/HCl and ion exchangers. The reported yields are unsatisfactory.
to The condensation in the presence of a catalyst system which consists of iron(II) chloride, metallic iron and HCl gas or aqueous solution is described in DOS 2160103 and US Patent 3789086. The formation of less by-products is advantageous compared with the aforementioned process using ZnCh/I-ICl.
However, corrosion problems and chloride contamination are equally disadvantageous.
An interesting alternative for the condensation of TMHQ with IP to d,l-a-tocopherol comprises using trifluoroacetic acid or its anhydride as the 2o catalyst (EP 12824). Although in this process the avoidance of HCl is achieved, the catalyst is relatively expensive.
The use of the heteropoly acid 12-tungstophosphoric or 12-tungstosilicic acid as the catalyst for the condensation of TMHQ with IP was described for the first time in React. Kinet. Catal. Lett. 47(1), 59-64 (1992). d,l-a-Tocopherol could be obtained, using various solvents, in about 90% yield.
A further process described in the literature [EP 658552; Bull. Chem.
Soc. Japan 68, 3569-3571 (1995)] for the synthesis of d,l-a-tocopherol is based on the use of a scandium, yttrium or lanthanide fluorosulphonate, nitrate or sulphate, e.g. scandium trifluoromethanesulphonate. With up to about 10%
excess of IP this process gives yields up to 98%.
The use of ion-exchanged bentonite, montmorillonite or saponite through treatment with e.g. scandium chloride and other metal salts (yttrium, lanthanum, etc.) as the catalyst for the condensation of TMHQ with IP or PH
has as a disadvantage the need for a large amount of catalyst [EP 677520;
Bull. Chem. Soc. Japan 69, 137-139 (1996)].
According to the Examples of EP 694 541 the condensation of TMHQ
with IP to a-tocopherol can be achieved in high yields and with a high product purity when such solvents as carbonate esters, fatty acid esters and mixed solvent systems are employed, catalysis being effected by ZnClzlHCl.
Disadvantages in this process are, in addition to the contamination of the waste water by zinc ions, the usual large "catalyst amount" of ZnCl2 used.
According to WO 97/28151 the acid-catalysed condensation of TMHQ
with IP can be performed in a cyclic carbonate or a-lactone as the solvent.
The preferred catalyst is a mixture of ortho boric acid and oxalic, tartaric or citric acid, or boron trifluoride etherate.
From the forgoing explanations it is evident that most of the previously 2o known processes have considerable disadvantages. Thus, corrosion problems occur in all processes in which such acid catalysts as boron trifluoride are used. Toxicity problems with the boron trifluoride adducts also occur, and when iron or zinc is used there is a contamination of the waste water with the metal ions which is today no longer acceptable. In some processes the formation of undesired by-products, e.g. phytyltoluene and chlorophytols, is an especially serious problem.
The object of the present invention is to provide a process for the manufacture of d,l-a-tocopherol by the condensation of trimethylhydroquinone 3o with isophytol or phytol in the presence of a catalyst and in a solvent which does not have the disadvantages of previously known procedures. In this respect, it is necessary that the catalyst used has no, or at least a much reduced, corrosive action, is non-toxic, does not contaminate the environment and catalyzes the desired reaction as selectively as possible and in high yields.
Furthermore, the catalyst should display its activity in small, really catalytic, amounts and should be readily separable and re-usable several times.
This object of the present invention is achieved by carrying out the condensation of trimethylhydroquinone with isophytol o.r phytol in the presence of at most 0.4 weight percent, based on the weight of isophytol or phytol, of 12-tungstophosphoric acid (H3PWlz04o), 12-molybdophosphoric acid (H3PMo,2040) or 12-tungstosilicic acid (H4S1W,ZO4o) as the catalyst. Moreover, the condensation is effected in ethylene or propylene carbonate or a mixture of both carbonates, or in a mixture of one or both of the carbonates and a non-polar solvent, as the solvent or solvent system, as appropriate.
The condensation itself is represented in the following Reaction Scheme, 15 showing the reaction with IP only.
Ho OH
OH
trimethylhydroquinone isophytol catalyst ~ -Hz0 HO
O
d,l-a-tocopherol Accordingly, the process in accordance with the invention for the manu-2o facture of d,l-a-tocopherol by the acid-catalyzed condensation of trimethylhy-droquinone with isophytol or phytol in ethylene or propylene carbonate or a mixture of both carbonates, or in a mixture of one or both of the carbonates and a non-polar solvent, is characterized by carrying out the condensation in the presence of at most 0.4 weight percent, based on the weight of isophytol or phytol, of 12-tungstophosphoric acid, 12-molybdophosphoric acid or 12-tungstosilicic acid as the acid catalyst.
If in addition to ethylene or propylene carbonate or a mixture of both carbonates a non-polar solvent is employed, this is suitably hexane, heptane or octane, preferably heptane.
The condensation is conveniently effected at temperatures from about 50°C to about 150°C, preferably from about 70°C to about 130°C, especially at about 100°C.
Furthermore, trimethylhydroquinone is conveniently used in a molar excess of about 30 to 120%, preferably about 50 to 100%, over the amount of 15 isophytol or phytol used. A particular range is about 30 to 65% molar excess.
The advantage of using a relatively large (up to about 120%) molar excess of trimethylhydroquinone is that an efficient process operation involves a continuous recycling of the unreacted trimethylhydroquinone into the reaction medium.
The amount of acid catalyst is conveniently about 0.1 to 0.4 weight percent, preferably about 0.35 weight percent, based on the weight of isophytol or phytol.
2s If the reaction is carried out in the presence of both a carbonate (ethylene or propylene carbonate, or both) and a non-polar solvent, then the volume ratio of the non-polar solvent to the carbonate used in the two-phase solvent system is conveniently in the range from 0.3:1 to 5:1, preferably from 1:1 to 3:2. The (total) amount of solvent, i.e. carbonate(s) and optionally also 3o non-polar solvent, is such that conveniently about 10 to 100 ml, preferably about 50 to 80 ml, for example about 30 to 60 ml, of carbonates) are used per 100 mmol of trimethylhydroquinone, and an additional about 10 to 150 ml, preferably about 25 to 100 ml, of non-polar solvent are used per 100 mmol of _7_ isophytol or phytol. In any event, only the one or the other carbonate is preferably used, either as the sole solvent or as the carbonate component of the solvent system with the non-polar solvent. As the latter, heptane is preferably employed, and the carbonate itself is preferably ethylene carbonate.
Moreover, the condensation is conveniently carried out under an inert gas atmosphere, preferably gaseous nitrogen or argon.
As the acid catalyst there is preferably used 12-tungstophosphoric acid or 12-tungstosilicic acid.
The process in accordance with the invention can be carried out ope-rationally in a very simple manner by adding isophytol or phytol or a solution thereof in the optionally employed non-polar solvent dropwise to a solution or ~5 suspension of the trimethylhydroquinone and the acid catalyst in ethylene or propylene carbonate or a mixture of both carbonates. The rate at which the isophytol or phytol is added is not critical. Conveniently, however, it or the solution thereof is added dropwise over a period of 0.1 to 3, preferably 0.3 to 2.0, hours. After completion of the isophytol or phytol addition and an 2o appropriate subsequent condensation, during which it is advantageous to remove the resulting water by azeotropic distillation or in the flow of inert gas used, isolation and purification of the obtained d,l-a-tocopherol can be effected by procedures conventionally used in organic chemistry, e.g. by distillation.
The process can be carried out batchwise or continuously.
Particular advantages in the use of the acid catalyst in the process in accordance with the invention are, in addition to high yields of d,l-a-tocopherol, the avoidance of corrosion, the avoidance of waste water contamination with heavy metal ions, the high selectivity as well as the 3o enabled ready isolation of the produced d,l-a-tocopherol from the mixture after reaction.
_g_ The process in accordance with the invention is illustrated by the following Examples:
Examples 1-22 To a mixture of 23.3 g (150 mmol) of 2,3,5-trimethylhydroquinone (98%
pure), 80 ml of ethylene carbonate or propylene carbonate (99% pure) and 150 mg of the heteropoly acid, 31.21 g (100 mmol) of isophytol (95% pure) either alone or in solution in up to 100 ml of heptane (or hexane or octane) were 1o added dropwise under an argon atmosphere and with stirring at 70°C
to 140°C, according to solvent, over a period of 20 to 120 minutes ("feed IP"). Du-ring the addition of isophytol an azeotropic mixture of water/heptane (or water/hexane or water/octane) was separated with the help of a water separator. After completion of the addition, the reaction mixture was heated ~5 under stirring at 140°C for another 30 minutes. The resulting two-phase system was cooled to 80°C and 100 ml of heptane (or hexane or octane) were added. The phases were separated and the carbonate layer was re-used. The heptane (or hexane or octane) layer was concentrated under reduced pressure to afford d,l-a-tocopherol as a brown oil. The results of the various trials are 2o summarized in the following Tables 1 and 2.
Table l: Condensation reaction between TMHf~,I and IP catalyzed by different heteropoly acids.
25 Ex. solvent catalyst react temp. feed IP yield purity (g /100 g product) (°C) (min.) (%)a %)b 1 EC HPW (0.35) 140 30 92.0 88.4 2 EC HPW (0.35) 140 60 93.4 90.9 30 EC HPW (0.35) 140 90 94.4 93.0 4 EC HPW (0.35) 140 120 95.3 91.3 5 PC HPW (1.13) 140 30 94.4 85.5 6 EC+Hep HPW (0.35) 100 20 96.4 92.1 7 EC+Hep HPW (0.35) 100 30 95.1 87.8 8 EC+Hep HPW (0.35) 100 60 95.7 91.3 9 EC+Hep HPW (0.35) 100 90 96.0 90.7 EC+Hep HPW (0.35) 100 120 97.6 91.8 s EC+Hep HSiW (0.35) 100 20 96.6 91.8 12 EC+Hep HPMo (0.35) 100 20 94.1 89.4 aisolated yield (not optimized, bdetermined by gas-liquid chromatographical (GLC) analysis of the isolated products (int. standard), EC=ethylene 1o carbonate, PC=propylene carbonate, Hep=heptane (in each case 100 ml used), HPW=H3PW,204o, HSiW=H4SiW1204o, HPMo=H3PMo,2040.
Table 2: Condensation reaction between TMHQ and IP catalyzed by HPW with different amounts of non-polar solvent (in each case feed IP = 30 min.) 1s Ex. non-polar ml* react. temp yield (%)a purity (%)b solvent (°C) 13 - 0 140 92.0 88.4 14 hexane 25 70 95.4 92.0 15 hexane 50 70 94.8 92.0 16 hexane 100 70 97.0 91.4 17 heptane 25 100 93.4 89.0 18 heptane 50 100 96.8 89.0 2s 19 heptane 100 100 96.4 92.1 20 octane 25 127 93.0 85.7 21 octane 50 127 94.1 87.0 22 octane 100 127 93.2 83.9 *based on 100 mmol TMHQ, aisolated yield (not optimized), bdetermined by GLC analysis of the isolated products (int. standard).
has as a disadvantage the need for a large amount of catalyst [EP 677520;
Bull. Chem. Soc. Japan 69, 137-139 (1996)].
According to the Examples of EP 694 541 the condensation of TMHQ
with IP to a-tocopherol can be achieved in high yields and with a high product purity when such solvents as carbonate esters, fatty acid esters and mixed solvent systems are employed, catalysis being effected by ZnClzlHCl.
Disadvantages in this process are, in addition to the contamination of the waste water by zinc ions, the usual large "catalyst amount" of ZnCl2 used.
According to WO 97/28151 the acid-catalysed condensation of TMHQ
with IP can be performed in a cyclic carbonate or a-lactone as the solvent.
The preferred catalyst is a mixture of ortho boric acid and oxalic, tartaric or citric acid, or boron trifluoride etherate.
From the forgoing explanations it is evident that most of the previously 2o known processes have considerable disadvantages. Thus, corrosion problems occur in all processes in which such acid catalysts as boron trifluoride are used. Toxicity problems with the boron trifluoride adducts also occur, and when iron or zinc is used there is a contamination of the waste water with the metal ions which is today no longer acceptable. In some processes the formation of undesired by-products, e.g. phytyltoluene and chlorophytols, is an especially serious problem.
The object of the present invention is to provide a process for the manufacture of d,l-a-tocopherol by the condensation of trimethylhydroquinone 3o with isophytol or phytol in the presence of a catalyst and in a solvent which does not have the disadvantages of previously known procedures. In this respect, it is necessary that the catalyst used has no, or at least a much reduced, corrosive action, is non-toxic, does not contaminate the environment and catalyzes the desired reaction as selectively as possible and in high yields.
Furthermore, the catalyst should display its activity in small, really catalytic, amounts and should be readily separable and re-usable several times.
This object of the present invention is achieved by carrying out the condensation of trimethylhydroquinone with isophytol o.r phytol in the presence of at most 0.4 weight percent, based on the weight of isophytol or phytol, of 12-tungstophosphoric acid (H3PWlz04o), 12-molybdophosphoric acid (H3PMo,2040) or 12-tungstosilicic acid (H4S1W,ZO4o) as the catalyst. Moreover, the condensation is effected in ethylene or propylene carbonate or a mixture of both carbonates, or in a mixture of one or both of the carbonates and a non-polar solvent, as the solvent or solvent system, as appropriate.
The condensation itself is represented in the following Reaction Scheme, 15 showing the reaction with IP only.
Ho OH
OH
trimethylhydroquinone isophytol catalyst ~ -Hz0 HO
O
d,l-a-tocopherol Accordingly, the process in accordance with the invention for the manu-2o facture of d,l-a-tocopherol by the acid-catalyzed condensation of trimethylhy-droquinone with isophytol or phytol in ethylene or propylene carbonate or a mixture of both carbonates, or in a mixture of one or both of the carbonates and a non-polar solvent, is characterized by carrying out the condensation in the presence of at most 0.4 weight percent, based on the weight of isophytol or phytol, of 12-tungstophosphoric acid, 12-molybdophosphoric acid or 12-tungstosilicic acid as the acid catalyst.
If in addition to ethylene or propylene carbonate or a mixture of both carbonates a non-polar solvent is employed, this is suitably hexane, heptane or octane, preferably heptane.
The condensation is conveniently effected at temperatures from about 50°C to about 150°C, preferably from about 70°C to about 130°C, especially at about 100°C.
Furthermore, trimethylhydroquinone is conveniently used in a molar excess of about 30 to 120%, preferably about 50 to 100%, over the amount of 15 isophytol or phytol used. A particular range is about 30 to 65% molar excess.
The advantage of using a relatively large (up to about 120%) molar excess of trimethylhydroquinone is that an efficient process operation involves a continuous recycling of the unreacted trimethylhydroquinone into the reaction medium.
The amount of acid catalyst is conveniently about 0.1 to 0.4 weight percent, preferably about 0.35 weight percent, based on the weight of isophytol or phytol.
2s If the reaction is carried out in the presence of both a carbonate (ethylene or propylene carbonate, or both) and a non-polar solvent, then the volume ratio of the non-polar solvent to the carbonate used in the two-phase solvent system is conveniently in the range from 0.3:1 to 5:1, preferably from 1:1 to 3:2. The (total) amount of solvent, i.e. carbonate(s) and optionally also 3o non-polar solvent, is such that conveniently about 10 to 100 ml, preferably about 50 to 80 ml, for example about 30 to 60 ml, of carbonates) are used per 100 mmol of trimethylhydroquinone, and an additional about 10 to 150 ml, preferably about 25 to 100 ml, of non-polar solvent are used per 100 mmol of _7_ isophytol or phytol. In any event, only the one or the other carbonate is preferably used, either as the sole solvent or as the carbonate component of the solvent system with the non-polar solvent. As the latter, heptane is preferably employed, and the carbonate itself is preferably ethylene carbonate.
Moreover, the condensation is conveniently carried out under an inert gas atmosphere, preferably gaseous nitrogen or argon.
As the acid catalyst there is preferably used 12-tungstophosphoric acid or 12-tungstosilicic acid.
The process in accordance with the invention can be carried out ope-rationally in a very simple manner by adding isophytol or phytol or a solution thereof in the optionally employed non-polar solvent dropwise to a solution or ~5 suspension of the trimethylhydroquinone and the acid catalyst in ethylene or propylene carbonate or a mixture of both carbonates. The rate at which the isophytol or phytol is added is not critical. Conveniently, however, it or the solution thereof is added dropwise over a period of 0.1 to 3, preferably 0.3 to 2.0, hours. After completion of the isophytol or phytol addition and an 2o appropriate subsequent condensation, during which it is advantageous to remove the resulting water by azeotropic distillation or in the flow of inert gas used, isolation and purification of the obtained d,l-a-tocopherol can be effected by procedures conventionally used in organic chemistry, e.g. by distillation.
The process can be carried out batchwise or continuously.
Particular advantages in the use of the acid catalyst in the process in accordance with the invention are, in addition to high yields of d,l-a-tocopherol, the avoidance of corrosion, the avoidance of waste water contamination with heavy metal ions, the high selectivity as well as the 3o enabled ready isolation of the produced d,l-a-tocopherol from the mixture after reaction.
_g_ The process in accordance with the invention is illustrated by the following Examples:
Examples 1-22 To a mixture of 23.3 g (150 mmol) of 2,3,5-trimethylhydroquinone (98%
pure), 80 ml of ethylene carbonate or propylene carbonate (99% pure) and 150 mg of the heteropoly acid, 31.21 g (100 mmol) of isophytol (95% pure) either alone or in solution in up to 100 ml of heptane (or hexane or octane) were 1o added dropwise under an argon atmosphere and with stirring at 70°C
to 140°C, according to solvent, over a period of 20 to 120 minutes ("feed IP"). Du-ring the addition of isophytol an azeotropic mixture of water/heptane (or water/hexane or water/octane) was separated with the help of a water separator. After completion of the addition, the reaction mixture was heated ~5 under stirring at 140°C for another 30 minutes. The resulting two-phase system was cooled to 80°C and 100 ml of heptane (or hexane or octane) were added. The phases were separated and the carbonate layer was re-used. The heptane (or hexane or octane) layer was concentrated under reduced pressure to afford d,l-a-tocopherol as a brown oil. The results of the various trials are 2o summarized in the following Tables 1 and 2.
Table l: Condensation reaction between TMHf~,I and IP catalyzed by different heteropoly acids.
25 Ex. solvent catalyst react temp. feed IP yield purity (g /100 g product) (°C) (min.) (%)a %)b 1 EC HPW (0.35) 140 30 92.0 88.4 2 EC HPW (0.35) 140 60 93.4 90.9 30 EC HPW (0.35) 140 90 94.4 93.0 4 EC HPW (0.35) 140 120 95.3 91.3 5 PC HPW (1.13) 140 30 94.4 85.5 6 EC+Hep HPW (0.35) 100 20 96.4 92.1 7 EC+Hep HPW (0.35) 100 30 95.1 87.8 8 EC+Hep HPW (0.35) 100 60 95.7 91.3 9 EC+Hep HPW (0.35) 100 90 96.0 90.7 EC+Hep HPW (0.35) 100 120 97.6 91.8 s EC+Hep HSiW (0.35) 100 20 96.6 91.8 12 EC+Hep HPMo (0.35) 100 20 94.1 89.4 aisolated yield (not optimized, bdetermined by gas-liquid chromatographical (GLC) analysis of the isolated products (int. standard), EC=ethylene 1o carbonate, PC=propylene carbonate, Hep=heptane (in each case 100 ml used), HPW=H3PW,204o, HSiW=H4SiW1204o, HPMo=H3PMo,2040.
Table 2: Condensation reaction between TMHQ and IP catalyzed by HPW with different amounts of non-polar solvent (in each case feed IP = 30 min.) 1s Ex. non-polar ml* react. temp yield (%)a purity (%)b solvent (°C) 13 - 0 140 92.0 88.4 14 hexane 25 70 95.4 92.0 15 hexane 50 70 94.8 92.0 16 hexane 100 70 97.0 91.4 17 heptane 25 100 93.4 89.0 18 heptane 50 100 96.8 89.0 2s 19 heptane 100 100 96.4 92.1 20 octane 25 127 93.0 85.7 21 octane 50 127 94.1 87.0 22 octane 100 127 93.2 83.9 *based on 100 mmol TMHQ, aisolated yield (not optimized), bdetermined by GLC analysis of the isolated products (int. standard).
Examples 23-28 To a mixture of 23.3 g (150 mmol) of 2,3,5-trimethylhydroquinone, 98%
pure), 80 ml of ethylene carbonate (99% pure), 25 to 100 ml of hexane or heptane and 150 mg of 12-tungstophosphoric acid, 31.21 g (100 mmol) of isophytol (95%) were added dropwise under stirring at 70°C or 100°C over a period of 30 minutes. After completion of the addition, the reaction mixture was stirred at this temperature for another 30 minutes while removing the heptane (or hexane). The resulting two-phase-system was cooled to 80°C
(or l0 60°C) and 100 ml of heptane (or hexane) were added. The phases were separated and the carbonate layer was re-used. The heptane (or hexane) layer was concentrated under reduced pressure to afford d,l-a-tocopherol as a brown oil. The results of the various trials are summarized in the following Table 3.
Table 3: Condensation reaction between TMHQ and IP catalyzed by HPW
whereby IP is added without solvent Ex. non-polar ml" react. temp. yield (%)a purity (%)b solvent (°C) 23 hexane 25 70 96.1 91.3 24 hexane 50 70 96.8 92.0 hexane 100 70 96.5 91.6 26 heptane 25 100 93.8 88.2 25 27 heptane 50 100 96.3 88.3 28 heptane 100 100 96.9 89.3 * based on 100 mmol TMHQ, aisolated yield (not optimized), bdetermined by GLC analysis of the isolated products (int. standard).
pure), 80 ml of ethylene carbonate (99% pure), 25 to 100 ml of hexane or heptane and 150 mg of 12-tungstophosphoric acid, 31.21 g (100 mmol) of isophytol (95%) were added dropwise under stirring at 70°C or 100°C over a period of 30 minutes. After completion of the addition, the reaction mixture was stirred at this temperature for another 30 minutes while removing the heptane (or hexane). The resulting two-phase-system was cooled to 80°C
(or l0 60°C) and 100 ml of heptane (or hexane) were added. The phases were separated and the carbonate layer was re-used. The heptane (or hexane) layer was concentrated under reduced pressure to afford d,l-a-tocopherol as a brown oil. The results of the various trials are summarized in the following Table 3.
Table 3: Condensation reaction between TMHQ and IP catalyzed by HPW
whereby IP is added without solvent Ex. non-polar ml" react. temp. yield (%)a purity (%)b solvent (°C) 23 hexane 25 70 96.1 91.3 24 hexane 50 70 96.8 92.0 hexane 100 70 96.5 91.6 26 heptane 25 100 93.8 88.2 25 27 heptane 50 100 96.3 88.3 28 heptane 100 100 96.9 89.3 * based on 100 mmol TMHQ, aisolated yield (not optimized), bdetermined by GLC analysis of the isolated products (int. standard).
Claims (14)
1. A process for the manufacture of d,l-.alpha.-tocopherol by the acid-catalyzed condensation of trimethylhydroquinone with isophytol or phytol in ethylene or propylene carbonate or a mixture of both carbonates or in a mixture of one or both of the carbonates and a non-polar solvent, which process is characterized by carrying out the condensation in the presence of at most 0.4 weight percent, based on the weight of isophytol or phytol, of 12-tungstophosphoric acid, 12-molybdophosphoric acid or 12-tungstosilicic acid as the acid catalyst.
2. A process according to claim 1, wherein the acid catalyst is 12-tungstophosphoric acid or 12-tungstosilicic acid.
3. A process according to claim 1 or 2, wherein the amount of acid catalyst is about 0.1 to 0.4, preferably about 0.35 weight percent, based on the weight of isophytol or phytol.
4. A process according to any one of claims 1 to 3, wherein the condensation is carried out in ethylene carbonate or a mixture thereof with a non-polar solvent.
5. A process according to any one of claims 1 to 4, wherein the non-polar solvent is hexane, heptane or octane, preferably heptane.
6. A process according to any one of claims 1 to 5, wherein the volume ratio of the non-polar solvent to carbonate in the two-phase solvent system is in the range from 0.3:1 to 5:1, preferably from 1:1 to 3:2..
7. A process according to any one of claims 1 to 6, wherein the condensation is effected at temperatures from about 50°C to about 150°C, preferably from about 70°C to about 130°C, especially at about 100°C.
8. A process according to any one of claims 1 to 7, wherein trimethyl-hydroquinone is used in a molar excess over isophytol or phytol of about 30 to 120%, preferably about 50 to 100%.
9. A process according to claim 8, wherein the molar excess is about 30 to 65%.
10. A process according to any one of claims 1 to 9, wherein about 10 to 100 ml, preferably about 50 to 80 ml, of carbonate(s) are used per 100 mmol of trimethylhydroquinone and, if a non-polar solvent is also used, about 10 to ml, preferably about 25 to 100 ml, of the non-polar solvent are used per 100 mmol of isophytol or phytol.
11. A process according to claim 10, wherein about 30 to 60 ml of carbonate(s) are used per 100 mmol of trimethylhydroquinone.
12. A process according to any one of claims 1 to 11, wherein isophytol or phytol or a solution thereof in the employed non-polar solvent is added dropwise to a solution or suspension of trimethylhydroquinone and the acid catalyst in ethylene or propylene carbonate or a mixture of both carbonates.
13. A process according to any one of claims 1 to 12, wherein the water resulting in the condensation is removed by azeotropic distillation or in the flow of inert gas used.
14. A process according to any one of claims 1 to 13, wherein the process is carried out batchwise or continuously.
Applications Claiming Priority (2)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| EP98112842 | 1998-07-10 | ||
| EP98112842.4 | 1998-07-10 |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CA2276921A1 true CA2276921A1 (en) | 2000-01-10 |
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ID=8232254
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA002276921A Abandoned CA2276921A1 (en) | 1998-07-10 | 1999-07-06 | Manufacture of d,1-alpha-tocopherol |
Country Status (8)
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|---|---|
| US (1) | US6452023B1 (en) |
| JP (1) | JP2000044556A (en) |
| KR (1) | KR20000011530A (en) |
| CN (1) | CN1245399C (en) |
| BR (1) | BR9902781A (en) |
| CA (1) | CA2276921A1 (en) |
| DE (1) | DE69920586T2 (en) |
| IN (1) | IN188479B (en) |
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| US6930191B2 (en) | 2002-10-10 | 2005-08-16 | Cognis Corporation | Methods of preparing tocopherol compound salts in supercritical media |
| KR20180050818A (en) * | 2016-11-07 | 2018-05-16 | 박종세 | The remote water level control apparatus of a multipurpose drainage device |
| EP3837248B1 (en) * | 2018-08-17 | 2024-07-24 | Basf Se | Synthesis of chromanol and 2-methyl-1,4-naphthoquinone derivatives |
| EP3837247B1 (en) * | 2018-08-17 | 2024-06-05 | Basf Se | Synthesis of chromanol derivatives |
| CN111646968B (en) * | 2020-05-28 | 2022-04-22 | 万华化学集团股份有限公司 | Method for preparing vitamin E |
| CN116987057A (en) * | 2023-06-16 | 2023-11-03 | 江苏宏邦化工科技有限公司 | Synthesis method of vitamin E acetate |
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| US5663376A (en) | 1994-07-27 | 1997-09-02 | Eisai Co., Ltd. | Process for the preparation of α-tocopherol |
| WO1997028151A1 (en) | 1996-01-29 | 1997-08-07 | Basf Aktiengesellschaft | METHOD OF PRODUCING DL-α-TOCOPHEROL OR DL-α-TOCOPHERYL ACETATE |
-
1999
- 1999-06-07 IN IN716MA1999 patent/IN188479B/en unknown
- 1999-06-26 DE DE69920586T patent/DE69920586T2/en not_active Expired - Lifetime
- 1999-06-29 US US09/342,272 patent/US6452023B1/en not_active Expired - Lifetime
- 1999-07-06 CA CA002276921A patent/CA2276921A1/en not_active Abandoned
- 1999-07-07 KR KR1019990027181A patent/KR20000011530A/en not_active Application Discontinuation
- 1999-07-08 BR BR9902781-0A patent/BR9902781A/en not_active Application Discontinuation
- 1999-07-08 JP JP11194076A patent/JP2000044556A/en not_active Withdrawn
- 1999-07-09 CN CNB991104226A patent/CN1245399C/en not_active Expired - Lifetime
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| US6452023B1 (en) | 2002-09-17 |
| DE69920586D1 (en) | 2004-11-04 |
| CN1241566A (en) | 2000-01-19 |
| KR20000011530A (en) | 2000-02-25 |
| BR9902781A (en) | 2000-05-16 |
| JP2000044556A (en) | 2000-02-15 |
| CN1245399C (en) | 2006-03-15 |
| IN188479B (en) | 2002-09-28 |
| DE69920586T2 (en) | 2005-11-03 |
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